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大脑中动脉闭塞后大鼠脑内MAP1B和MAP2的上调:年龄的影响

Upregulation of MAP1B and MAP2 in the rat brain after middle cerebral artery occlusion: effect of age.

作者信息

Popa-Wagner A, Schröder E, Schmoll H, Walker L C, Kessler C

机构信息

Department of Neurology, University of Greifswald, Germany.

出版信息

J Cereb Blood Flow Metab. 1999 Apr;19(4):425-34. doi: 10.1097/00004647-199904000-00008.

Abstract

Although stroke in humans usually afflicts the elderly, most experimental studies on the nature of cerebral ischemia have used young animals. This is especially important when studying restorative processes that are age dependent. To explore the potential of older animals to initiate regenerative processes after cerebral ischemia, the authors studied the expression of the juvenile-specific cytoskeletal protein, microtubule-associated protein (MAP) 1B, and the adult-specific protein, MAP2, in male Sprague-Dawley rats at 3 months and 20 months of age. The levels of MAP1B and MAP2 transcripts and the corresponding proteins declined with increasing age in the hippocampus. In the cortex, the levels of the transcripts did not change significantly with age, but the morphologic features of immunostained fibers were clearly affected by age; that is, cortical MAP1B fibers became thicker, and MAP2 fibers, more diffuse, in aged rats. Focal cerebral ischemia, produced by reversible occlusion of the right middle cerebral artery, resulted in a large decrease in the expression of both MAP1B and MAP2 in the infarct core at the messenger ribonucleic acid and protein levels. However, at 1 week after the stroke, there was vigorous expression of MAP1B and its messenger ribonucleic acid, as well as MAP2 protein, in the border zone adjacent to the infarct of 3-month-old and 20 month-old male Sprague-Dawley rats. The upregulation of these key cytologic elements generally was diminished in aged rats compared with young animals, although the morphologic features of fibers in the infarct border zone were similar in both age groups. These results suggest that the regenerative potential of the aged rat brain appears to be competent, although attenuated, at least with respect to MAP1B and MAP2 expression up to 20 months of age.

摘要

虽然人类中风通常多见于老年人,但大多数关于脑缺血本质的实验研究都使用了幼龄动物。在研究与年龄相关的恢复过程时,这一点尤为重要。为了探究老年动物在脑缺血后启动再生过程的潜力,作者研究了幼年特异性细胞骨架蛋白微管相关蛋白(MAP)1B和成年特异性蛋白MAP2在3月龄和20月龄雄性Sprague-Dawley大鼠中的表达情况。海马体中MAP1B和MAP2转录本及相应蛋白的水平随年龄增长而下降。在皮质中,转录本水平并未随年龄显著变化,但免疫染色纤维的形态特征明显受年龄影响;也就是说,老年大鼠皮质中的MAP1B纤维变粗,而MAP2纤维更加弥散。通过可逆性阻断右侧大脑中动脉造成局灶性脑缺血,导致梗死核心区MAP1B和MAP2在信使核糖核酸和蛋白水平的表达大幅下降。然而,在中风后1周,3月龄和20月龄雄性Sprague-Dawley大鼠梗死灶相邻的边缘区有强烈的MAP1B及其信使核糖核酸以及MAP2蛋白的表达。与幼龄动物相比,老年大鼠中这些关键细胞学成分的上调通常有所减弱,尽管两个年龄组梗死边缘区纤维的形态特征相似。这些结果表明,至少在20月龄前,老年大鼠脑的再生潜力似乎仍然存在,尽管有所减弱,至少在MAP1B和MAP2表达方面是这样。

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